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神经氨酸酶-3是淋巴细胞功能相关抗原-1黏附的负调节因子。

Neuraminidase-3 Is a Negative Regulator of LFA-1 Adhesion.

作者信息

Howlader Md Amran, Li Caishun, Zou Chunxia, Chakraberty Radhika, Ebesoh Njuacha, Cairo Christopher W

机构信息

Department of Chemistry, University of Alberta, Edmonton, AB, Canada.

出版信息

Front Chem. 2019 Nov 22;7:791. doi: 10.3389/fchem.2019.00791. eCollection 2019.

Abstract

Within the plasma membrane environment, glycoconjugate-receptor interactions play an important role in the regulation of cell-cell interactions. We have investigated the mechanism and activity of the human neuraminidase (NEU) isoenzyme, NEU3, on T cell adhesion receptors. The enzyme is known to prefer glycolipid substrates, and we confirmed that exogenous enzyme altered the glycolipid composition of cells. NEU3 was able to modify the sialic acid content of purified LFA-1 . Enzymatic activity of NEU3 resulted in re-organization of LFA-1 into large clusters on the membrane. This change was facilitated by an increase in the lateral mobility of LFA-1 upon NEU3 treatment. Changes to the lateral mobility of LFA-1 were specific for NEU3 activity, and we observed no significant change in diffusion when cells were treated with a bacterial NEU (NanI). Furthermore, we found that NEU3 treatment of cells increased surface expression levels of LFA-1. We observed that NEU3-treated cells had suppressed LFA-1 adhesion to an ICAM-1 coated surface using an static adhesion assay. These results establish that NEU3 can modulate glycoconjugate composition and contribute to the regulation of integrin activity. We propose that NEU3 should be investigated to determine its role on LFA-1 within the inflammatory cascade.

摘要

在质膜环境中,糖缀合物 - 受体相互作用在细胞间相互作用的调节中发挥着重要作用。我们研究了人类神经氨酸酶(NEU)同工酶NEU3对T细胞黏附受体的作用机制和活性。已知该酶偏好糖脂底物,并且我们证实外源性酶改变了细胞的糖脂组成。NEU3能够改变纯化的淋巴细胞功能相关抗原-1(LFA-1)的唾液酸含量。NEU3的酶活性导致LFA-重组为膜上的大簇。NEU3处理后LFA-1侧向流动性的增加促进了这种变化。LFA-1侧向流动性的变化对NEU3活性具有特异性,并且当用细菌神经氨酸酶(NanI)处理细胞时,我们未观察到扩散有显著变化。此外,我们发现用NEU3处理细胞会增加LFA-1的表面表达水平。我们通过静态黏附试验观察到,用NEU3处理的细胞抑制了LFA-1与细胞间黏附分子-1(ICAM-1)包被表面的黏附。这些结果表明,NEU3可以调节糖缀合物组成,并有助于整合素活性的调节。我们建议对NEU3进行研究,以确定其在炎症级联反应中对LFA-1的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4cb2/6882948/c6270eab0662/fchem-07-00791-g0001.jpg

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